Frontiers in Genetics (Jan 2021)

Characteristics of Genetic Variations Associated With Lennox-Gastaut Syndrome in Korean Families

  • Jin Ok Yang,
  • Jin Ok Yang,
  • Min-Hyuk Choi,
  • Min-Hyuk Choi,
  • Ji-Yong Yoon,
  • Jeong-Ju Lee,
  • Sang Ook Nam,
  • Soo Young Jun,
  • Hyeok Hee Kwon,
  • Sohyun Yun,
  • Su-Jin Jeon,
  • Su-Jin Jeon,
  • Iksu Byeon,
  • Debasish Halder,
  • Juhyun Kong,
  • Byungwook Lee,
  • Jeehun Lee,
  • Joon-Won Kang,
  • Nam-Soon Kim,
  • Nam-Soon Kim

DOI
https://doi.org/10.3389/fgene.2020.590924
Journal volume & issue
Vol. 11

Abstract

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Lennox-Gastaut syndrome (LGS) is a severe type of childhood-onset epilepsy characterized by multiple types of seizures, specific discharges on electroencephalography, and intellectual disability. Most patients with LGS do not respond well to drug treatment and show poor long-term prognosis. Approximately 30% of patients without brain abnormalities have unidentifiable causes. Therefore, accurate diagnosis and treatment of LGS remain challenging. To identify causative mutations of LGS, we analyzed the whole-exome sequencing data of 17 unrelated Korean families, including patients with LGS and LGS-like epilepsy without brain abnormalities, using the Genome Analysis Toolkit. We identified 14 mutations in 14 genes as causes of LGS or LGS-like epilepsy. 64 percent of the identified genes were reported as LGS or epilepsy-related genes. Many of these variations were novel and considered as pathogenic or likely pathogenic. Network analysis was performed to classify the identified genes into two network clusters: neuronal signal transmission or neuronal development. Additionally, knockdown of two candidate genes with insufficient evidence of neuronal functions, SLC25A39 and TBC1D8, decreased neurite outgrowth and the expression level of MAP2, a neuronal marker. These results expand the spectrum of genetic variations and may aid the diagnosis and management of individuals with LGS.

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